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通过离心和表面固定化在三维多孔基质中创建生长因子梯度。

Creating growth factor gradients in three dimensional porous matrix by centrifugation and surface immobilization.

机构信息

Department of Advanced Materials, Hannam University, 461-6 Jeonmin Dong, Yuseong Gu, Daejeon 305-811, Republic of Korea.

出版信息

Biomaterials. 2011 Nov;32(32):8254-60. doi: 10.1016/j.biomaterials.2011.07.027. Epub 2011 Jul 27.

Abstract

Polycaprolactone (PCL)/Pluronic F127 cylindrical scaffolds with gradually increasing growth factor concentrations were fabricated by the centrifugation of fibril-like PCLs and the subsequent fibril surface immobilization of growth factors. The cylindrical scaffolds exhibited gradually increasing surface areas along the longitudinal direction [from 3.17 ± 0.05 m(2)/g (top position) to 5.42 ± 0.01 m(2)/g (bottom position)]. The growth factors (BMP-7, TGF-β(2) and VEGF(165)) as model bioactive molecules were immobilized onto the fibril surfaces of the scaffolds via heparin binding to produce scaffolds with gradually increasing concentrations of growth factors from the top position (BMP-7, 60.89 ± 2.51; TGF-β(2), 42.85 ± 2.00; VEGF(165), 42.52 ± 3.22 ng/scaffold section) to the bottom position (BMP-7, 181.07 ± 3.21; TGF-β(2), 142.08 ± 2.91; VEGF(165), 112.00 ± 4.00 ng/scaffold section). The released amount of growth factor (VEGF(165)) from the cylindrical scaffold gradually decreased along the longitudinal direction in a sustained manner for up to 35 days, which can allow for a minutely controlled spatial distribution of growth factors in a 3D environment. The 3D porous scaffold with a concentration gradient of growth factors may become a useful tool for basic studies, including in vitro investigations of 3D chemotaxis/haptotaxis for the control of specific biological process. It may also be used as a tissue engineering scaffolding system for a variety of tissues/organs requiring the spatial regulation of growth factors for effective regeneration.

摘要

聚己内酯 (PCL)/Pluronic F127 圆柱支架通过纤维状 PCL 的离心和随后的生长因子纤维表面固定化来制备,其具有沿纵向逐渐增加的表面积[从顶部位置的 3.17±0.05 m(2)/g (顶部位置)到底部位置的 5.42±0.01 m(2)/g (底部位置)]。生长因子 (BMP-7、TGF-β(2) 和 VEGF(165)) 作为模型生物活性分子通过肝素结合固定在支架的纤维表面上,从而产生具有从顶部位置 (BMP-7,60.89±2.51; TGF-β(2),42.85±2.00; VEGF(165),42.52±3.22 ng/支架段) 到底部位置 (BMP-7,181.07±3.21; TGF-β(2),142.08±2.91; VEGF(165),112.00±4.00 ng/支架段) 的生长因子浓度逐渐增加的支架。生长因子 (VEGF(165)) 从圆柱支架中的释放量在长达 35 天的时间内沿纵向持续逐渐减少,这可以允许在 3D 环境中精细控制生长因子的空间分布。具有生长因子浓度梯度的 3D 多孔支架可能成为一种有用的工具,用于基础研究,包括用于控制特定生物过程的 3D 趋化性/趋触性的体外研究。它也可以用作组织工程支架系统,用于各种需要空间调节生长因子以实现有效再生的组织/器官。

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